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嵌入非污损环境中的不同细胞外基质模拟肽序列对人皮肤角质形成细胞和成纤维细胞在可变形基质上特异性黏附的影响。

Influence of different ECM mimetic peptide sequences embedded in a nonfouling environment on the specific adhesion of human-skin keratinocytes and fibroblasts on deformable substrates.

作者信息

Salber Jochen, Gräter Stefan, Harwardt Marc, Hofmann Matthias, Klee Doris, Dujic Jadranka, Jinghuan Huang, Ding Jiandong, Kippenberger Stefan, Bernd August, Groll Jürgen, Spatz Joachim P, Möller Martin

机构信息

DWI an der RWTH Aachen e.V. Pauwelsstr. 8, 52074 Aachen, Germany.

出版信息

Small. 2007 Jun;3(6):1023-31. doi: 10.1002/smll.200600596.

DOI:10.1002/smll.200600596
PMID:17455182
Abstract

Mechanical stress is a decisive factor for the differentiation, proliferation, and general behavior of cells. However, the specific signaling of mechanotransduction is not fully understood. One basic problem is the clear distinction between the different extracellular matrix (ECM) constituents that participate in cellular adhesion and their corresponding signaling pathways. Here, a system is proposed that enables mechanical stimulation of human-skin-derived keratinocytes and human dermal fibroblasts that specifically interact with peptide sequences immobilized on a non-interacting but deformable substrate. The peptide sequences mimic fibronectin, laminin, and collagen type IV, three major components of the ECM. To achieve this, PDMS is activated using ammonia plasma and coated with star-shaped isocyanate-terminated poly(ethylene glycol)-based prepolymers, which results in a functional coating that prevents unspecific cell adhesion. Specific cell adhesion is achieved by functionalization of the layers with the peptide sequences in different combinations. Moreover, a method that enables the decoration of deformable substrates with cell-adhesion peptides in extremely defined nanostructures is presented. The distance and clustering of cell adhesion molecules below 100 nm has been demonstrated to be of utmost importance for cell adhesion. Thus we present a new toolbox that allows for the detailed analysis of the adhesion of human-skin-derived cells on structurally and biochemically decorated deformable substrates.

摘要

机械应力是细胞分化、增殖及一般行为的决定性因素。然而,机械转导的具体信号传导尚未完全明确。一个基本问题是,参与细胞黏附的不同细胞外基质(ECM)成分与其相应信号通路之间的明确区分。在此,我们提出了一种系统,该系统能够对人皮肤来源的角质形成细胞和人真皮成纤维细胞进行机械刺激,这些细胞可与固定在非相互作用但可变形基质上的肽序列特异性相互作用。这些肽序列模拟了ECM的三种主要成分:纤连蛋白、层粘连蛋白和IV型胶原蛋白。为实现这一点,使用氨等离子体对聚二甲基硅氧烷(PDMS)进行活化,并涂覆以星形异氰酸酯封端的聚乙二醇基预聚物,从而形成一种功能性涂层,可防止非特异性细胞黏附。通过用不同组合的肽序列对这些层进行功能化处理来实现特异性细胞黏附。此外,还介绍了一种能够在极其精确的纳米结构中用细胞黏附肽修饰可变形基质的方法。已证明细胞黏附分子低于100纳米的间距和聚集对于细胞黏附至关重要。因此,我们展示了一个新的工具箱,可用于详细分析人皮肤来源的细胞在结构和生化修饰的可变形基质上的黏附情况。

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